银屑病
免疫学
免疫系统
树突状细胞
调解人
白细胞介素17
T细胞
医学
内分泌学
作者
Takeshi Nakahara,Makiko Kido‐Nakahara,Fumitaka Ohno,Dugarmaa Ulzii,Takahito Chiba,Gaku Tsuji,Masutaka Furue
出处
期刊:Allergy
[Wiley]
日期:2017-09-28
卷期号:73 (2): 511-515
被引量:38
摘要
Abstract Endothelin‐1 ( ET ‐1) is associated with skin diseases such as atopic dermatitis ( AD ) and psoriasis. ET ‐1 is enhanced in the skin of patients AD and psoriasis. In addition, plasma levels of ET ‐1 are elevated in AD and psoriasis. Although both AD and psoriasis are T‐cell–mediated skin diseases, the association between ET ‐1 and the T‐cell immune response has not been clarified. To evaluate the role of ET ‐1 in inflammatory skin disease, we sought to investigate the effects of ET ‐1 on the functions of dendritic cells ( DC s) and subsequent immune responses. For this purpose, we immunohistochemically confirmed the upregulation of ET ‐1 in the epidermis of patients with AD or psoriasis. ET ‐1 directly induced phenotypic maturation of bone marrow‐derived DC s ( BMDC s). In addition, ET ‐1 augmented the production of several cytokines and allogeneic stimulatory capacity of BMDC s. Interestingly, ET ‐1–activated BMDC s primed T cells to produce Th1 and Th17 cytokines, but not Th2 cytokines. These findings indicate that ET ‐1 polarizes the DC –T‐cell response toward Th17/1 differentiation and may augment the persistent course of inflammatory skin diseases.
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